Adamas Pharmaceuticals, Inc. (Nasdaq: ADMS), a company dedicated
to developing and delivering medicines that make a meaningful
difference to people affected by neurological diseases, today
announced five posters will be presented at the International
Parkinson and Movement Disorder Society (MDS) Virtual Congress,
taking place September 17 – 22, 2021. The poster presentations will
focus on GOCOVRI® (amantadine) extended-release capsules, the first
and only FDA-approved medicine indicated for the treatment of
dyskinesia in patients with Parkinson’s disease receiving
levodopa-based therapy, with or without concomitant dopaminergic
medications, and as an adjunctive treatment to levodopa/carbidopa
in patients with Parkinson’s disease experiencing OFF episodes.
“We are pleased to present several analyses of different
published clinical studies to highlight the importance of choosing
the appropriate treatment options to address motor complications in
Parkinson’s disease. GOCOVRI’s clinical results continue to
demonstrate its unique and meaningful treatment impact on both OFF
and dyskinesia – including through indirect comparisons with other
levodopa-adjunctive treatments and amantadine-based products,” said
Adrian Quartel, M.D., Chief Medical Officer, Adamas. “Additionally,
in a post-hoc analysis, GOCOVRI as an only/early add-on treatment
to levodopa showed reductions of OFF and dyskinesia that were
similar to, or greater than, those seen in the overall trial
population. Overall, we are pleased to offer patients a
non-surgical treatment option that increases their GOOD ON time and
doesn’t necessitate a trade-off between treating OFF or
dyskinesia.”
One presentation (Poster 446) will highlight pooled data from
GOCOVRI pivotal trials to evaluate the efficacy of GOCOVRI as a
first/early add-on treatment to levodopa for Parkinson’s disease
(PD) motor complications (OFF or dyskinesia). This post-hoc
analysis examined two subgroups of patients: 1) those using
levodopa as their only medication for PD, and 2) those who
developed motor complications and entered the GOCOVRI trials within
five years of being diagnosed with PD. The results of this analysis
support GOCOVRI as an early adjunctive treatment to levodopa for
patients with early motor complications - OFF or dyskinesia.
Two presentations will highlight indirect treatment comparisons
between GOCOVRI and other treatment options based on existing
published clinical data, that support GOCOVRI as a highly
differentiated, cost-effective treatment option:
- Poster 500: In a comparison of efficacy data from pivotal
clinical trials for approved levodopa-adjunctive treatments,
GOCOVRI and deep brain stimulation (DBS) reduced OFF time and
dyskinesia by over 30% relative to placebo. Oral dopaminergic
treatments and levodopa/carbidopa intestinal gel (CLIG) reduced OFF
time by 15-29% over placebo, with a 12-31% increase in dyskinesia
for the oral treatments, and no significant impact on dyskinesia
for CLIG.
- Poster 520: The efficacy of GOCOVRI versus other formulations
of amantadine were compared through a traditional Indirect
Treatment Comparison (ITC) analysis. While GOCOVRI has shown
statistically significant reductions in both OFF time, by 36%, and
dyskinesia, by 27%, amantadine immediate release (IR) and
amantadine IR/extended release (IR/ER) reduced dyskinesia scores by
19% and 13%, respectively. Neither amantadine IR nor amantadine
IR/ER demonstrated a significant change in OFF time in randomized,
double-blind, clinical trials.
Two additional posters will be presented that support the use of
GOCOVRI to manage motor complications and their impact on daily
activities in people with PD:
- Poster 395: For patients who may be candidates for device-aided
therapies to manage motor complications (DBS, levodopa/carbidopa
intestinal gel, or subcutaneous-apomorphine infusion), a post-hoc
analysis showed GOCOVRI increased GOOD ON time by ~2.8 hours vs.
placebo, with corresponding reductions in OFF time and dyskinesia.
These results suggest GOCOVRI should be considered for certain
patients who may be otherwise eligible for device-aided
therapies.
- Poster 414: This post-hoc analysis of clinical trial data
evaluates the collective interference of dyskinesia and OFF across
daily activities and experiences for persons with Parkinson’s and
shows that GOCOVRI significantly reduced dyskinesia and OFF and
their associated impact on these daily activities.
The posters will be available for on-demand viewing beginning
September 10, 2021, and available for the duration of the meeting.
Details are as follows:
Poster 395: Should amantadine DR/ER be considered prior
to device-aided therapies for Parkinson’s disease? Lead
author: Robert A. Hauser, M.D., University of South Florida
Abstract Category: Clinical Trials
Poster 414: Amantadine DR/ER-related reduction in OFF and
dyskinesia improved patient-rated interference with activities and
social interactions Lead author: Kelly E. Lyons, Ph.D.,
University of Kansas Medical Center Abstract Category:
Clinical Trials
Poster 446: Amantadine DR/ER efficacy as early add-on for
motor complications in Parkinson’s disease Lead author:
Caroline M. Tanner, M.D., Ph.D., University of California, San
Francisco Abstract Category: Clinical Trials
Poster 500: Indirect treatment comparison of adjunctive
treatments for patients with Parkinson’s disease experiencing motor
complications Lead author: Daniel E. Kremens, M.D., J.D.,
Jefferson University Hospital, Philadelphia, PA Abstract
Category: Pharmacology and Therapy
Poster 520: Analysis of amantadine formulations for OFF
and dyskinesia in Parkinson disease Lead author: Wolfgang
Oertel, M.D., Ph.D., University of Marburg, Germany Abstract
Category: Pharmacology and Therapy
About Parkinson’s Disease, dyskinesia and OFF
Parkinson’s disease (PD) is a progressive, neurodegenerative
disorder caused by the gradual loss of brain cells that produce the
neurotransmitter dopamine and affects approximately one million
people in the United States. Dopamine decline in the brain results
in a wide range of motor (movement-related) and non-motor symptoms.
As the disease progresses, people taking levodopa-based therapy are
likely to experience reemergence or sudden return of stiffness,
rigidity and tremors between medication doses, referred to as OFF
episodes, which may be unpredictable. The primary treatment for PD
is with levodopa; however, over time levodopa may lead to
involuntary, uncontrolled movements known as dyskinesia. The abrupt
and unpredictable transitions between episodes of dyskinesia,
normal movement, and OFF lead to considerable impact on patients’
lives.
About GOCOVRI
GOCOVRI® (amantadine) extended-release capsules is the first and
only FDA-approved medicine indicated for the treatment of
dyskinesia in patients with Parkinson’s disease receiving
levodopa-based therapy, with or without concomitant dopaminergic
medications, and as an adjunctive treatment to levodopa/carbidopa
in patients with Parkinson’s disease experiencing OFF episodes.
Taken once daily at bedtime, GOCOVRI provides an initial lag
(delayed release) and a slow rise in amantadine concentration
during the night, resulting in a high concentration from the
morning and throughout the waking day (extended release).
Additionally, in the clinical trials, the adjunctive use of GOCOVRI
did not require dose changes to dopaminergic therapies. The most
commonly observed adverse reactions with GOCOVRI were
hallucinations, dizziness, dry mouth, peripheral edema,
constipation, falls and orthostatic hypotension.
For more information about GOCOVRI, please visit
www.GOCOVRI.com.
IMPORTANT SAFETY INFORMATION
CONTRAINDICATIONS
GOCOVRI is contraindicated in patients with creatinine clearance
below 15 mL/min/1.73 m2
WARNINGS AND PRECAUTIONS
Falling Asleep During Activities of Daily Living and Somnolence:
Patients treated with Parkinson’s disease medications have reported
falling asleep during activities of daily living. If a patient
develops daytime sleepiness during activities that require full
attention (e.g., driving a motor vehicle, conversations, eating),
GOCOVRI should ordinarily be discontinued or the patient should be
advised to avoid potentially dangerous activities.
Suicidality and Depression: Monitor patients for depression,
including suicidal ideation or behavior. Prescribers should
consider whether the benefits outweigh the risks of treatment with
GOCOVRI in patients with a history of suicidality or
depression.
Hallucinations/Psychotic Behavior: Patients with a major
psychotic disorder should ordinarily not be treated with GOCOVRI
because of the risk of exacerbating psychosis. Observe patients for
the occurrence of hallucinations throughout treatment, especially
at initiation and after dose increases.
Dizziness and Orthostatic Hypotension: Monitor patients for
dizziness and orthostatic hypotension, especially after starting
GOCOVRI or increasing the dose.
Withdrawal-Emergent Hyperpyrexia and Confusion: Rapid dose
reduction or abrupt discontinuation of GOCOVRI, may cause an
increase in the symptoms of Parkinson’s disease or cause delirium,
agitation, delusions, hallucinations, paranoid reaction, stupor,
anxiety, depression, or slurred speech. Avoid sudden
discontinuation of GOCOVRI.
Impulse Control/Compulsive Behaviors: Patients may experience
urges (e.g. gambling, sexual, money spending, binge eating) and the
inability to control them. It is important for prescribers to ask
patients or their caregivers about the development of new or
increased urges. Consider dose reduction or stopping
medications.
ADVERSE REACTIONS
The most common adverse reactions (>10%) were hallucination,
dizziness, dry mouth, peripheral edema, constipation, fall, and
orthostatic hypotension.
Please see full Prescribing Information for additional important
safety information at
https://www.gocovri.com/assets/pdfs/Gocovri_Prescribing_Information.pdf.
About Adamas
At Adamas our vision is clear – to deliver innovative medicines
that reduce the burden of neurological diseases on patients,
caregivers and society. We are a fully-integrated company focused
on growing a portfolio of therapies to address a range of
neurological diseases. For more information, please visit
www.adamaspharma.com.
View source
version on businesswire.com: https://www.businesswire.com/news/home/20210916005353/en/
Media: Sarah Mathieson Vice President of Corporate
Communications 510-450-3528 smathieson@adamaspharma.com
Investors: Peter Vozzo Westwicke 443-213-0505
peter.vozzo@westwicke.com
Adamas Pharmaceuticals (NASDAQ:ADMS)
Historical Stock Chart
From Oct 2024 to Nov 2024
Adamas Pharmaceuticals (NASDAQ:ADMS)
Historical Stock Chart
From Nov 2023 to Nov 2024
